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一种非肽类 Mas 受体激动剂 AVE-0991 对糖尿病大鼠心肾保护作用的可能机制。

Possible mechanism of the cardio-renal protective effects of AVE-0991, a non-peptide Mas-receptor agonist, in diabetic rats.

机构信息

ISF College of Pharmacy, Moga, India.

出版信息

J Renin Angiotensin Aldosterone Syst. 2012 Sep;13(3):334-40. doi: 10.1177/1470320311435534. Epub 2012 Feb 17.

DOI:10.1177/1470320311435534
PMID:22345112
Abstract

HYPOTHESIS

This study was designed to investigate the cardio-renal protective effect of AVE-0991, a non-peptide Mas-receptor agonist, and A-779, a Mas-receptor antagonist, in diabetic rats.

MATERIALS AND METHODS

Wistar rats treated with streptozotocin (50 mg/kg, i.p., once), developed diabetes mellitus after 1 week. After 8 weeks, myocardial functions were assessed by measuring left ventricular developed pressure (LVDP), rate of left ventricular pressure development (dp/dt (max)), rate of left ventricular pressure decay (dp/dt (min)) and left ventricular end diastolic pressure (LVEDP) on an isolated Langendorff's heart preparation. Further, mean arterial blood pressure (MABP) was measured by using the tail-cuff method. Assessment of renal functions and lipid profile was carried out using a spectrophotometer.

RESULTS

The administration of streptozotocin to rats produced persistent hyperglycaemia, dyslipidaemia and hypertension which consequently produced cardiac and renal dysfunction in 8 weeks. AVE0991 treatment produced cardio-renal protective effects, as evidenced by a significant increase in LVDP, dp/dt (max), dp/dt (min) and a significant decrease in LVEDP, BUN, and protein urea. Further, AVE-0991 treatment for the first time has been shown to reduce dyslipidaemia and produced antihyperglycaemic activity in streptozotocin-treated rats. However, MABP and creatinine clearance remained unaffected with AVE-0991 treatment.

CONCLUSIONS

AVE-0991 produced cardio-renal protection possibly by improving glucose and lipid metabolism in diabetic rats, independent of its blood pressure lowering action.

摘要

假设

本研究旨在探讨非肽类 Mas 受体激动剂 AVE-0991 和 Mas 受体拮抗剂 A-779 对糖尿病大鼠的心脏-肾脏保护作用。

材料和方法

Wistar 大鼠经链脲佐菌素(50mg/kg,ip,单次)处理后,1 周后发展为糖尿病。8 周后,通过测量左心室发展压(LVDP)、左心室压力发展率(dp/dt(max))、左心室压力衰减率(dp/dt(min))和左心室舒张末期压(LVEDP),在离体 Langendorff 心脏制剂上评估心肌功能。进一步,通过尾套法测量平均动脉血压(MABP)。使用分光光度计评估肾功能和血脂谱。

结果

链脲佐菌素给药导致大鼠持续高血糖、血脂异常和高血压,进而在 8 周内导致心脏和肾脏功能障碍。AVE0991 治疗产生了心脏-肾脏保护作用,表现为 LVDP、dp/dt(max)、dp/dt(min)显著增加,LVEDP、BUN 和蛋白尿素显著降低。此外,AVE-0991 治疗首次显示可降低血脂异常,并在链脲佐菌素处理的大鼠中产生抗高血糖作用。然而,AVE-0991 治疗对 MABP 和肌酐清除率没有影响。

结论

AVE-0991 通过改善糖尿病大鼠的葡萄糖和脂质代谢产生心脏-肾脏保护作用,而不依赖于其降压作用。

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